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Antifungal Activity of the Biphosphinic Cyclopalladate C7a against Candida albicans Yeast Forms In Vitro and In Vivo

Julian E Muñoz 1, 2
Diego C P Rossi 1
Kelly Ishida 1
Cristina C Spadari 1
Marcia S. C. Melhem 3
Daniel M Garcia 4
Antonio C. F. Caires 5
Carlos P. Taborda 1, 6
Elaine G. Rodrigues 7
2
 
Faculty of Health Sciences, Colegio Mayor de Cundinamarca University, Bogotá, Colombia
3
 
Parasitology Section, Technical Division of Medical Biology, Instituto Adolfo Lutz, São Paulo, Brazil
5
 
Interdisciplinary Center for Biochemical Investigation, University of Mogi das Cruzes, Mogi das Cruzes, Brazil
Publication typeJournal Article
Publication date2017-05-03
scimago Q1
wos Q1
SJR1.172
CiteScore8.5
Impact factor4.5
ISSN1664302X
Microbiology (medical)
Microbiology
Abstract
Vulvovaginal and invasive candidiasis are frequent conditions in immunosuppressed individuals caused by Candida albicans and non-albicans Candida spp. Fluconazole and Amphotericin B are the main drugs used to fight the infection. However, resistance to fluconazole and other azole antifungal drugs is an important clinical problem that encourages the search for new therapeutic alternatives. In this work, we evaluate the antifungal activity of the biphosphinic cyclopalladate C7a in the in vitro and in vivo model. Our results showed fungicidal activity, with low values of minimal inhibitory concentrations and minimum fungicidal concentrations, even for fluconazole and/or miconazole resistant Candida isolates. Fluorescence microscopy and transmission electron microscopy revealed that the compound was able to inhibit the formation of hyphae/pseudohyphae and, moreover, promoted morphological alterations in cellular organelles and structures, such as disruption of cell wall, apparent mitochondrial swelling, chromatin marginalization into the nuclei and increased numbers of electron-lucent vacuoles. C7a significantly decreased the biofilm formation and reduced the viability of yeast cells in mature biofilms when tested against a virulent C. albicans strain. In vivo assays demonstrated a significant decrease of fungal burden in local (vaginal canal) and disseminated (kidneys) infection. In addition, we observed a significant increase in the survival of the systemically-infected animals treated with C7a. Our results suggest C7a as a novel therapeutic agent for vaginal and disseminated candidiasis, and an alternative for conventional drug-resistant Candida.
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GOST Copy
Muñoz J. E. et al. Antifungal Activity of the Biphosphinic Cyclopalladate C7a against Candida albicans Yeast Forms In Vitro and In Vivo // Frontiers in Microbiology. 2017. Vol. 8.
GOST all authors (up to 50) Copy
Muñoz J. E., Rossi D. C. P., Ishida K., Spadari C. C., Melhem M. S. C., Garcia D. M., Caires A., Taborda C. P., Rodrigues E. G. Antifungal Activity of the Biphosphinic Cyclopalladate C7a against Candida albicans Yeast Forms In Vitro and In Vivo // Frontiers in Microbiology. 2017. Vol. 8.
RIS |
Cite this
RIS Copy
TY - JOUR
DO - 10.3389/fmicb.2017.00771
UR - https://doi.org/10.3389/fmicb.2017.00771
TI - Antifungal Activity of the Biphosphinic Cyclopalladate C7a against Candida albicans Yeast Forms In Vitro and In Vivo
T2 - Frontiers in Microbiology
AU - Muñoz, Julian E
AU - Rossi, Diego C P
AU - Ishida, Kelly
AU - Spadari, Cristina C
AU - Melhem, Marcia S. C.
AU - Garcia, Daniel M
AU - Caires, Antonio C. F.
AU - Taborda, Carlos P.
AU - Rodrigues, Elaine G.
PY - 2017
DA - 2017/05/03
PB - Frontiers Media S.A.
VL - 8
PMID - 28515716
SN - 1664-302X
ER -
BibTex
Cite this
BibTex (up to 50 authors) Copy
@article{2017_Muñoz,
author = {Julian E Muñoz and Diego C P Rossi and Kelly Ishida and Cristina C Spadari and Marcia S. C. Melhem and Daniel M Garcia and Antonio C. F. Caires and Carlos P. Taborda and Elaine G. Rodrigues},
title = {Antifungal Activity of the Biphosphinic Cyclopalladate C7a against Candida albicans Yeast Forms In Vitro and In Vivo},
journal = {Frontiers in Microbiology},
year = {2017},
volume = {8},
publisher = {Frontiers Media S.A.},
month = {may},
url = {https://doi.org/10.3389/fmicb.2017.00771},
doi = {10.3389/fmicb.2017.00771}
}